We utilized the C2 symmetric diene-diol 2 as the starting material, and the skeleton of ent-brevipolide H (ent-1) was prepared by the sequence of cross metathesis, cyclopropanation, Sharpless asymmetric α-hydroxylation and ring-closing-metathesis. The anti-addition of the sulfur ylide to the α,β-unsaturated enone 5 was be developed to generate the key cyclopropane moiety, whose stereochemistry was lated confirmrd by X-ray crystallography. The substrates with different hydroxyl protecting groups, i.e. ethoxymethyl ether and acetonide, lead to the different stereo-assignment of the cyclopropane. The first total synthesis of ent-brevipolide H (ent-1) was achieved after the linkage of 4-methoxycinnamic acid to an ester, the formation of 5,6-dihydro-2-pyrone and deprotection.